Journal of medicinal and pharmaceutical chemistry 2008-07-24

Identification of a potent, selective, and orally active leukotriene a4 hydrolase inhibitor with anti-inflammatory activity.

Cheryl A Grice, Kevin L Tays, Brad M Savall, Jianmei Wei, Christopher R Butler, Frank U Axe, Scott D Bembenek, Anne M Fourie, Paul J Dunford, Katherine Lundeen, Fawn Coles, Xiaohua Xue, Jason P Riley, Kacy N Williams, Lars Karlsson, James P Edwards

Index: J. Med. Chem. 51 , 4150-69, (2008)

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Abstract

LTA 4H is a ubiquitously distributed 69 kDa zinc-containing cytosolic enzyme with both hydrolase and aminopeptidase activity. As a hydrolase, LTA 4H stereospecifically catalyzes the transformation of the unstable epoxide LTA 4 to the diol LTB 4, a potent chemoattractant and activator of neutrophils and a chemoattractant of eosinophils, macrophages, mast cells, and T cells. Inhibiting the formation of LTB 4 is expected to be beneficial in the treatment of inflammatory diseases such as inflammatory bowel disease (IBD), asthma, and atherosclerosis. We developed a pharmacophore model using a known inhibitor manually docked into the active site of LTA 4H to identify a subset of compounds for screening. From this work we identified a series of benzoxazole, benzthiazole, and benzimidazole inhibitors. SAR studies resulted in the identification of several potent inhibitors with an appropriate cross-reactivity profile and excellent PK/PD properties. Our efforts focused on further profiling JNJ 27265732, which showed encouraging efficacy in a disease model relevant to IBD.

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